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非人灵长类动物子宫内膜中雌激素、孕激素和雄激素受体的激素调节与定位:孕激素受体拮抗剂的作用

Hormonal regulation and localization of estrogen, progestin and androgen receptors in the endometrium of nonhuman primates: effects of progesterone receptor antagonists.

作者信息

Slayden Ov D, Brenner Robert M

机构信息

Division of Reproductive Sciences, Oregon National Primate Research Center, 505 NW 185th Ave, Beaverton, OR 97006, USA.

出版信息

Arch Histol Cytol. 2004 Dec;67(5):393-409. doi: 10.1679/aohc.67.393.

Abstract

This article reviews the effects of estradiol (E(2)), progesterone (P) and P receptor antagonists (PA) on the rhesus macaque endometrium. Ovariectomized macaques can be treated with implants of estradiol (E(2)) and P to induce precisely controlled, artificial menstrual cycles. During these cycles, treatment with E(2) alone induces an artificial proliferative phase marked by extensive endometrial epithelial cell proliferation and increased expression of stromal and epithelial estrogen receptor (ER) and P receptor (PR). Androgen receptor (AR) is also upregulated by E(2) but is expressed only by the endometrial stroma. Progesterone acts on the E(2) primed endometrium to induce secretory differentiation and causes suppression of epithelial and stromal ER, epithelial PR, and stromal AR in the functionalis zone. However, epithelial ER and PR are retained in the basalis zone during the secretory phase. When potent P antagonists (PA) are administered acutely at the end of an E(2) + P induced cycle, menses typically ensues similar to P withdrawal at the end of the menstrual cycle. When PAs are administered chronically there is significant blockage of all P- dependent effects including upregulation of ER, PR and AR and suppression of glandular secretory function. However, chronic PA administration also inhibits estrogen-dependent endometrial cell proliferation and growth. This endometrial antiproliferative effect is the basis of the clinical use of PA to control various diseases such as endometriosis.

摘要

本文综述了雌二醇(E₂)、孕酮(P)及孕酮受体拮抗剂(PA)对恒河猴子宫内膜的影响。切除卵巢的猕猴可用雌二醇(E₂)和孕酮植入物进行治疗,以诱导精确控制的人工月经周期。在这些周期中,单独使用E₂进行治疗会诱导一个人工增殖期,其特征为子宫内膜上皮细胞大量增殖,基质和上皮雌激素受体(ER)以及孕酮受体(PR)的表达增加。雄激素受体(AR)也会被E₂上调,但仅在内膜基质中表达。孕酮作用于经E₂预处理的子宫内膜,诱导分泌期分化,并导致功能层上皮和基质ER、上皮PR以及基质AR的表达受到抑制。然而,在分泌期,上皮ER和PR会保留在基底层。当在E₂ + P诱导周期结束时急性给予强效孕酮拮抗剂(PA)时,通常会出现月经,类似于月经周期结束时孕酮撤退的情况。当长期给予PA时,所有依赖孕酮的效应都会受到显著阻断,包括ER、PR和AR的上调以及腺分泌功能的抑制。然而,长期给予PA也会抑制雌激素依赖的子宫内膜细胞增殖和生长。这种子宫内膜抗增殖作用是PA在临床上用于控制诸如子宫内膜异位症等各种疾病的基础。

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